A liposome based platelet substitute, the plateletsome, with hemostatic efficacy.

M E Rybak, L A Renzulli
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引用次数: 67

Abstract

The complexity of platelet mediated hemostasis has hindered development of a platelet substitute for transfusion therapy. In the current study, the hemostatic efficacy of a liposome based modality, the plateletsome, is demonstrated. A deoxycholate extract of a platelet membrane fraction, with a minimum of 15 proteins including GPIb, GPIIb-IIIa and GPIV/III, was incorporated into sphingomyelin: phosphatidylcholine: monosialylganglioside or egg phosphatide small unilamellar vesicles by reverse-phase/sonication and French press extrusion. These plateletsomes decreased bleeding by 67% in the tail bleeding time in rats made thrombocytopenic (platelets < 30,000/microliters) with external irradiation (7-9Gy) by Cesium source. Efficacy was also demonstrated in the thrombocytopathic, Fawn-Hooded rat, but to a lesser extent than in the thrombocytopenic animals. Direct plateletsome infusion to the tail wound was more effective than systemic administration for all effective preparations. On post-mortem examination, no pathologic thrombi were detected by gross and histopathologic examination of the lungs, livers, kidneys, or spleens of thrombocytopenic or normal animals after plateletsome infusion. No evidence of intravascular coagulation, monitored by levels of circulating fibrinogen and platelet counts, was observed when plateletsomes were administered intravenously to rabbits. No deleterious effect, either inhibition or hyperaggregability, on platelet aggregation studies in vitro was observed. While further refinements are clearly required, this study indicates that liposomes bearing specific platelet proteins may provide a basis for a clinically applicable platelet substitute.

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一种基于脂质体的血小板替代物,血小板体,具有止血功效。
血小板介导止血的复杂性阻碍了血小板替代输血治疗的发展。在目前的研究中,一种基于脂质体的止血效果,血小板,被证明。血小板膜部分脱氧胆酸提取物,至少含有15种蛋白质,包括GPIb, GPIIb-IIIa和GPIV/III,通过反相/超声和法压挤压纳入鞘磷脂、磷脂酰胆碱、单唾液神经节苷脂或蛋磷脂小单层囊泡。这些血小板体在铯源外照射(7-9Gy)致血小板减少(血小板< 30,000/微升)大鼠尾出血时间内可减少出血67%。效果也证明了在血小板病变,小鹿兜帽大鼠,但在较小程度上比在血小板减少的动物。在所有有效制剂中,尾创面直接输注血小板比全身给药更有效。死后检查,血小板减少或正常动物输注血小板后肺、肝、肾、脾的大体和组织病理学检查均未发现病理性血栓。通过循环纤维蛋白原水平和血小板计数监测,当血小板体静脉注射给兔时,没有观察到血管内凝血的证据。在体外的血小板聚集研究中,没有观察到抑制或超聚集的有害作用。虽然还需要进一步的改进,但这项研究表明,含有特异性血小板蛋白的脂质体可能为临床应用的血小板替代品提供基础。
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